Targeting of the FYVE domain to endosomal membranes is regulated by a histidine switch

Lee, Stephanie A.; Eyeson, Rosemary; Cheever, Matthew L.; Geng, Jinming; Verkhusha, Vladislav V.; Burd, Christopher G.; Overduin, Michael; Kutateladze, Tatiana G.

doi:10.1073/pnas.0503900102

Cited by 96 publications

(96 citation statements)

References 44 publications

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“…Vps27p binds directly to endosomal lipid phosphatidylinositol 3-phosphate (PI(3)P) through its FYVE domain (a zinc finger domain highly conserved in Fab1p, YOTB, Vac1p, and EEA1 proteins (10)). In agreement with this, the interaction of the FYVE domain in the mammalian EEA1 protein with a PI(3)P lipid is pH-dependent (39). In wild-type cells, GFP-Vps27p-H190A/H191A, in which the His-190 and His-191 residues in the FYVE domain were replaced by Ala residues (39,40), was distributed in the cytoplasm at all pH levels (Fig.…”

Section: Endosomal Na ϩ /H ϩ Exchange Activity Is Required For Efficisupporting

confidence: 74%

“…In agreement with this, the interaction of the FYVE domain in the mammalian EEA1 protein with a PI(3)P lipid is pH-dependent (39). In wild-type cells, GFP-Vps27p-H190A/H191A, in which the His-190 and His-191 residues in the FYVE domain were replaced by Ala residues (39,40), was distributed in the cytoplasm at all pH levels (Fig. 6, C and D), indicating that the interaction of Vps27p with PI(3)P in the endosomal membrane via its FYVE domain is pH-dependent.…”

Section: Endosomal Na ϩ /H ϩ Exchange Activity Is Required For Efficisupporting

confidence: 67%

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The Endosomal Na+/H+ Exchanger Contributes to Multivesicular Body Formation by Regulating the Recruitment of ESCRT-0 Vps27p to the Endosomal Membrane

Mitsui

Koshimura

Yoshikawa

et al. 2011

Journal of Biological Chemistry

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Multivesicular bodies (MVBs) are late endosomal compartments containing luminal vesicles (MVB vesicles) that are formed by inward budding of the endosomal membrane. In budding yeast, MVBs are an important cellular mechanism for the transport of membrane proteins to the vacuolar lumen. This process requires a class E subset of vacuolar protein sorting (VPS) genes. VPS44 (allelic to NHX1) encodes an endosomelocalized Na ؉ /H ؉ exchanger. The function of the VPS44 exchanger in the context of vacuolar protein transport is largely unknown. Using a cell-free MVB formation assay system, we demonstrated that Nhx1p is required for the efficient formation of MVB vesicles in the late endosome. The recruitment of Vps27p, a class E Vps protein, to the endosomal membrane was dependent on Nhx1p activity and was enhanced by an acidic pH at the endosomal surface. Taken together, we propose that Nhx1p contributes to MVB formation by the recruitment of Vps27p to the endosomal membrane, possibly through Nhx1p antiporter activity.Multivesicular bodies (MVBs) 3 are a subset of late endosomes that contain internal vesicles, permitting precursor and plasma membrane proteins to reach the lysosome or vacuole lumen for degradation or maturation, respectively. In eukaryotic cells, the MVB pathway controls various important processes such as receptor down-regulation, antigen presentation, cytokinesis, retroviral budding, and autophagy (1-6). In the budding yeast Saccharomyces cerevisiae, previous studies identified a number of genes involved in vacuolar protein sorting (VPS) (7,8). These Vps proteins function at distinct steps of protein transport between the Golgi complex and the vacuole (7,8). A subset of Vps proteins, class E proteins, is involved in MVB formation. Most class E proteins are components of five distinct complexes; Vps27p-Hse1p (also called endosomal sorting complexes required for transport-0 (ESCRT-0), -I, -II, and -III and Vps4p. These complexes are required for the formation of internal vesicles and sorting of cargo proteins to the vesicles from the endosomal membrane (3, 9). Vps27p (ESCRT-0) recruits ESCRT-I, which in turn recruits and/or activates ESCRT-II and ESCRT-III at the endosome (3, 10). Recent in vitro studies have provided new insights into the precise role of each ESCRT complex in MVB formation (11-13). ESCRT-0 initiates the MVB sorting process by recruiting ESCRT-I to the endosomal membrane and concentrating ubiquitylated MVB cargos to the vesicle budding site (12). ESCRT-I and ESCRT-II are directly involved in membrane budding by stabilizing the bud necks, whereas ESCRT-III is responsible for the cleavage of bud necks (11-13). Finally, the AAA-type ATPase Vps4p dissociates the ESCRT-III complex from the endosome (14). The sequential activity of these complexes on the cytoplasmic surface of endosomes directs the budding and fission of vesicles into the lumen of the endosome and the sequestration of cargo proteins in the vesicle. Defects in ESCRT proteins prevent internal vesicle formation and result in exagg...

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Section: Endosomal Na ϩ /H ϩ Exchange Activity Is Required For Efficisupporting

confidence: 74%

Section: Endosomal Na ϩ /H ϩ Exchange Activity Is Required For Efficisupporting

confidence: 67%

The Endosomal Na+/H+ Exchanger Contributes to Multivesicular Body Formation by Regulating the Recruitment of ESCRT-0 Vps27p to the Endosomal Membrane

Mitsui

Koshimura

Yoshikawa

et al. 2011

Journal of Biological Chemistry

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“…5) (35,38,39). Consistent with our pulldown experiments, RME-8 K8A and RME-8 K25A co-localize with EEA1 to a similar extent as wild type RME-8 (Fig.…”

Section: Volume 290 • Number 35 • August 28 2015supporting

confidence: 77%

Receptor-mediated Endocytosis 8 Utilizes an N-terminal Phosphoinositide-binding Motif to Regulate Endosomal Clathrin Dynamics

Xhabija¹,

Vacratsis

2015

Journal of Biological Chemistry

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Background: RME-8 is involved in clathrin removal at early endosomes. Results: RME-8 possesses a novel PI(3)P-binding motif within its N terminus. Conclusion: Association of RME-8 with PI(3)P is required for endosomal clathrin removal and alters the steady state localization of retrograde transport cargo CI-MPR. Significance: Regulation of PI(3)P association or PI(3)P levels is likely critical for controlling early endosomal organizational activities.

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“…Docking of PtdIns(3,5)P 2 was only successful when H178 and H249 of KlHsv2 were protonated. This is reminiscent of the histidine switch observed for PtdIns3P binding of the EEA1-FYVE domain (47) and PtdIns(3,4,5)P 3 binding of the GRP1 PH domain (48). We thus speculate that PtdIns(3,5)P 2 binding might also depend on pH.…”

Section: Discussionmentioning

confidence: 95%

Structural and functional characterization of the two phosphoinositide binding sites of PROPPINs, a β-propeller protein family

Krick

Busse

Scacioc

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

160

234

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β-propellers that bind polyphosphoinositides (PROPPINs), a eukaryotic WD-40 motif-containing protein family, bind via their predicted β-propeller fold the polyphosphoinositides PtdIns3P and PtdIns(3,5) P 2 using a conserved FRRG motif. PROPPINs play a key role in macroautophagy in addition to other functions. We present the 3.0-Å crystal structure of Kluyveromyces lactis Hsv2, which shares significant sequence homologies with its three Saccharomyces cerevisiae homologs Atg18, Atg21, and Hsv2. It adopts a seven-bladed β-propeller fold with a rare nonvelcro propeller closure. Remarkably, in the crystal structure, the two arginines of the FRRG motif are part of two distinct basic pockets formed by a set of highly conserved residues. In comprehensive in vivo and in vitro studies of ScAtg18 and ScHsv2, we define within the two pockets a set of conserved residues essential for normal membrane association, phosphoinositide binding, and biological activities. Our experiments show that PROPPINs contain two individual phosphoinositide binding sites. Based on docking studies, we propose a model for phosphoinositide binding of PROPPINs.autophagy | protein-lipid interactions | X-ray crystallography | yeast

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Targeting of the FYVE domain to endosomal membranes is regulated by a histidine switch

Cited by 96 publications

References 44 publications

The Endosomal Na+/H+ Exchanger Contributes to Multivesicular Body Formation by Regulating the Recruitment of ESCRT-0 Vps27p to the Endosomal Membrane

The Endosomal Na+/H+ Exchanger Contributes to Multivesicular Body Formation by Regulating the Recruitment of ESCRT-0 Vps27p to the Endosomal Membrane

Receptor-mediated Endocytosis 8 Utilizes an N-terminal Phosphoinositide-binding Motif to Regulate Endosomal Clathrin Dynamics

Structural and functional characterization of the two phosphoinositide binding sites of PROPPINs, a β-propeller protein family

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